Naphthols useful in antiviral methods

ABSTRACT

The present invention relates to a novel class of compounds that are potent inhibitors of HIV reverse transcriptase and HIV integrase. In addition to being multienzyme inhibitors, the inventive compounds of the present invention are remarkable in at least two other respects. First, they do not appear to be toxic to cells at typical therapeutic concentrations. Second, they appear to be equally effective against mutant strains of HIV reverse transcriptase commonly found in patients who have developed resistance to current reverse transcriptase inhibitors. Because the inventive compounds show promise in combatting viral resistance and are potent inhibitors of both HIV reverse transcriptase and integrase, they are ideal candidates for use in combination with existing therapies or alone in treating AIDS or HIV infection.

This invention was made with Government support under Grant No. GM39552, awarded by the National Institute of Health. The Government has certain rights in this invention.

CROSS-REFERENCE TO RELATED APPLICATION

This is an application based on provisional patent application Ser. No. 60/045,583, filed May 5, 1997, now abandoned, and priority therefrom is hereby claimed.

FIELD OF THE INVENTION

The present invention generally relates to naphthols useful as dyes and color indicators, more particularly to naphthols with antiviral properties for applications in the fields of virology and molecular medicine, and more specifically, to novel compounds that reduce or inhibit the activities of two key enzymes in the HIV life cycle, reverse transcriptase and integrase.

BACKGROUND OF THE INVENTION

A great variety of naphthols are known and useful as dyes and color indicators. Among these are naphthalene sulfonic acid compounds such as calcomine orange, which has been taught useful as an inert background dye in assaying peroxidatively active substances by U.S. Pat. No. 5,089,420, issued Feb. 18, 1992, inventors Albarella et al. Calcomine orange has been reported (Available Chemicals Database) to have the asymmetrical structure shown by Compound A: ##STR1##

U.S. Pat. No. 5,589,510, issued Dec. 31, 1996, inventors Ono et al., disclose a method for inhibiting retroviral infection by administering a naphthalenesulfonic acid compound represented by the Compound B: ##STR2## wherein R¹¹ to R²⁷ are individually selected from the group consisting of hydrogen atom, hydroxyl group, amino group which is optionally substituted with alkyl or aryl groups, sulfo groups, carboxyl groups, amide group which is optionally substituted with alkyl or aryl groups, acylamino groups, sulfonamide groups, sulfonylamino groups, alkoxy groups and halogen atoms; provided that at least one of R¹¹ to R¹⁷ is hydroxyl or amino group, at least one of R²¹ to R²⁷ is hydroxyl or amino group, at least one of R¹¹ to R¹⁷ is sulfo group, and at least one of R²¹ to R²⁷ is sulfo group; A and B are individually selected from the group consisting of hydrogen atom, alkyl (C₁ -C₄) groups, alkoxy (C₁ -C₄) groups, and halogen atoms.

There have also been reported some naphthol compounds considered "confirmed active" in AIDS antiviral screens. These include calcomine scarlet 4BNC (CAS Registry No. 5893323), direct fast scarlet 4BSW (CAS Registry No. 6420446), and brilliant paper scarlet G (CAS Registry No. 6460011). However, these just noted naphthol dyes all contain three or more sulfonic acid groups. The calcomine scarlet 4BNC, for example, is 2-naphthalenesulfonic acid, 7-[(4-aminobenzoyyl)amino]-3-[[4-[(2,5-dichloro-4-sulfophenyl)azo]-2-ethoxy-6-sulfo-1-naphthalenyl]azo]-4-hydroxy-,trisodium salt (9CI).

Human immunodeficiency virus ("HIV"), a retrovirus in the lentivirus family, is believed to be the etiological agent of acquired immunodeficiency syndrome ("AIDS"). Chemotherapeutic strategies for treating AIDS or HIV infection have traditionally targeted critical enzymes in the viral life cycle. For example, HIV reverse transcriptase, which is necessary to convert the RNA-based viral genome to DNA, continues to be a target of drug therapy. More recently, the focus has shifted to multiple enzymatic targets such as the combination of reverse transcriptase and protease.

Currently used reverse transcriptase inhibitors fall into two categories. The nucleoside analogue inhibitors such as 3'-azido-3'-deoxythymidine ("AZT"), dideoxyinosine ("ddI"), and dideoxycytidine ("ddC") are deoxynucleoside mimics. These compounds are converted into triphosphate forms by intracellular enzymes and inhibit reverse transcriptase mediated DNA synthesis by acting as DNA chain terminators. However, presumably because of the cross reactivity with host polymerases, the side effects are notoriously severe and generally limit the therapeutic index of this class of drugs to relatively low levels.

The non-nucleoside inhibitors include nevirapine, tetrahydroimidazo-[4,5,1-jk] benzodiazepine-2(1H)-thione ("TIBO"), 1-[(2-hydroxyethoxy)-methyl]-6-(phenylthio)thimine ("HEPT"), and 2-pyridone derivatives. These compounds bind to an allosteric site on reverse transcriptase and are believed to inhibit the enzyme by affecting its conformational flexibility. Although this class of drugs has minimal side effects, because of the rapid development of viral resistance, these drugs become virtually ineffective typically within about six weeks.

In an effort to stem the development of viral resistance, combination therapies attacking multiple enzymatic targets have been recently advocated. For example, various protease inhibitors have been successfully combined with nucleoside inhibitors such as AZT and have reduced blood virus counts to virtually undetectable levels in some patients. However, this remarkable response is not reproduced in all patients. Moreover, in addition to the punishing side effects, users of protease inhibitors often must follow a demanding treatment regimen, with the risk that if a few doses are skipped, any advantage of the combination in stemming viral resistance may be lost.

The earlier noted U.S. Pat. No. 5,589,510 suggests use of its naphthalene sulfonic acid compounds in administration with other known HIV-reverse transcriptase inhibitors, such as AZT. Nevertheless, a need exists for new drugs against the HIV virus, particularly those that could be effective in inhibiting multiple enzymes necessary for the HIV virus. Ideally, these new drugs would only selectively target the virus and produce minimal patient side effects. Moreover, based upon the success of current combination therapies, the new drugs should be adaptable for use in such therapies by either attacking at novel targets for use with one or more existing drugs, or attacking multiple targets by themselves.

SUMMARY OF THE INVENTION

In one aspect of the present invention, novel naphthols are provided that are useful as dyes and color indicators. These novel compounds have been discovered to have anti-viral properties against retroviruses, particularly to be inhibitors of HIV reverse transcriptase and/or HIV integrase. It is particularly advantageous to have a drug with multiple sites of attack, such as to be an inhibitor of both reverse transcriptase and integrase, as here.

The inventive naphthols have the general formula:

    Ar--X--Ar'

wherein Ar is a naphthol substituted with anionic groups or groups readily converted to anionic groups, provided that there are no more than two sulfonic acid groups on the molecule, Ar' is a substituted or unsubstituted aryl (C₆ -C₁₂) or substituted or unsubstituted heteroaryl (C₁ -C₁₂), and X is a substantially rigid linker preferably attached via amide (or amide analogous) bonds. Amide analogous bonds include vinylogous amides. A particularly preferred linker is the urea linker (--N(CO)N--). However, other examples of suitable linkers include but are not limited to: --N(CS)N-- (thiourea); --N(CO)(CO)N-- (oxalyl); --N(CO)C(CO)N-- (malonyl); --N(CO)O-- (carbamate); and --N(CO)CH₂ CH₂ (CO)N-- (succinyl), as well as moieties with aromatic rings, squarates, and cage structures.

One group of preferred compounds of the present invention are of the formula: ##STR3## wherein R₁ and R₂ individually is selected from a group consisting of substituted aryl (C₆ -C₁₂), unsubstituted aryl (C₆ -C₁₂), substituted heteroaryl (C₁ -C₁₂) and unsubstituted heteroaryl (C₁ -C₁₂), which are bound via an azo or amide group, provided that neither R₁ nor R₂ contains a sulfonic acid group, Y and Y' each is an anionic moiety, such as sulfonic, carboxylic and tetrazol, or one readily converted to anionic, such as sulfonic acid ester and sulfonic acid thioester, and X is a linker as above described, which is bonded through amide or amide analogous bonds by a "J" or a "K" position link. "P" is one or more counterions, such as protons, alkali, metal, or alkaline earth cations.

For example, many of the preferred compounds with confirmed retroviral activity have the structure ##STR4## wherein Y, Y', and X are as already described, Z is an azo or amide linkage, and one or both of R₃ and R₄ include a readily ionizable group, such as a carboxyl, a trizol, or a tetrazol group.

Two examples of particularly preferred embodiments of the invention are the salts or protonated species: ##STR5##

The IC₅₀ for Compound 5 has been tested as 200 nM and that of Compound 159 at 220 nM. In cell-based anti-HIV (XTT) assays, Compound 5 was confirmed active.

In another aspect of the invention, methods for inhibiting HIV reverse transcriptase and/or integrase and methods for inhibiting HIV replication are provided that comprise administering an effective amount of at least one inventive compound or a salt thereof. Because the inventive compounds show promise in combating viral resistance and are potent inhibitors of both HIV reverse transcriptase and integrase, they are ideal candidates for use in combination with existing therapies or alone in treating AIDS or HIV infection.

In yet another aspect of the invention, pharmaceutical compositions are provided which comprise at least one inventive compound (or salt thereof) in association with a pharmaceutically acceptable carrier, diluent or excipient. Particularly preferred pharmaceutical compositions are formulated for topical application in treating retroviral diseases such as herpes simplex.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1 graphically illustrates the results of a reverse transcriptase (RT) assay for an embodiment of the invention designated "Compound 5;" and,

FIG. 2 graphically illustrates a cell-based anti-HIV (XTT) assay for the Compound 5 embodiment.

DETAILED DESCRIPTION OF THE INVENTION

Compounds of this invention are naphthols that may be used as dyes and color indicators; however, because these compounds have anti-viral properties against retroviruses they are contemplated for use in virology applications. In particular, the compounds are potent inhibitors of HIV reverse transcriptase and/or integrase.

The novel inhibitors of the present invention are a result of structure-based drug design efforts using the 2.8 Å crystal structure of HIV reverse transcriptase complexed to DNA. Small molecules were individually "docked" to binding sites in the enzyme and evaluated as potential lead compounds. So that the number of synthesized compounds is minimized, a database containing only commercially available compounds was used. An example of a database of this type is the Available Chemicals Database distributed by Molecular Design Limited (San Leandro, Calif.).

A lead compound that emerged was carbonyl-J ("Compound 1"). ##STR6## Carbonyl-J inhibited the activity of HIV reverse transcriptase with an IC₅₀ of approximately 5 micromolar ("μM"). IC₅₀ is the concentration at which the compound inhibits 50 percent of the enzyme's activity.

Continuing the strategy of minimum synthesis, the initial derivatives of carbonyl-J were found by searching the database of commercially available compounds. However, this time, instead of focusing on a particular compound's interaction with the enzyme, the search focused on structural similarity to carbonyl-J. A notable result from this effort was the identification of "calcomine orange" which was found by us to inhibit the HIV reverse transcriptase with an IC₅₀ of 1.5 μM. Although calcomine orange was purportedly a known compound, we found there to be ambiguity in its actual structure, as discussed below. Although calcomine orange has been known and used as a dye, it has not been known for biological properties.

The reported structure for calcomine orange was determined to be incorrect. According to the Available Chemicals Database, the structure of calcomine orange is asymmetrical, as shown by Compound A. ##STR7## However, based upon a series of NMR experiments, it has been discovered that the commercially available sample of calcomine orange is actually a symmetrical diphenyl species which lacks the reported carboxylic functionality, as shown by Compound C. It is possible that the asymmetrical Compound A structure was present as a contaminant in the commercially obtained source. ##STR8##

In addition to inhibiting reverse transcriptase which translates the viral RNA-based genome into DNA, carbonyl-J and the tested calcomine orange (Compound C) also inhibit HIV integrase. Also a critical enzyme, integrase is involved in two separate reactions and is so named because of its involvement in stably "integrating" viral DNA into host DNA. The first reaction is termed "3' processing" and is the transesterification of the 3' end of the viral DNA in the cytoplasm. The second is termed "strand transfer" and involves another transesterification reaction in the nucleus which attaches the 3' end of the viral DNA to host DNA. Notably both carbonyl-J and calcomine orange are also potent integrase inhibitors with IC₅₀ values of 2.5 μM and 2.0 μM, respectively, for both the 3' processing and strand transfer activities.

Using both carbonyl-J and calcomine orange as lead compounds, analogs that also inhibit reverse transcriptase and/or integrase were prepared.

In general, compounds of the present invention may be described by the formula:

    Ar--X--Ar'

wherein Ar is a naphthol substituted with an anionic moiety or with a group readily converted to an anionic moiety, such as an ester, provided that when the anionic group is sulfonic acid there are no more than two present and Ar' is a substituted or unsubstituted aryl (C₆ -C₁₂) or substituted or unsubstituted heteroaryl (C₁ -C₁₂) and X is a substantially rigid linker. Preferably Ar' is also a naphthol, and both Ar and Ar' are substituted with anionic moieties such as sulfonic, carboxylic, or tetrazol groups, or with an ester such as sulfonic acid ester and sulfonic acid thioester. Typical substituents are where there is an anionic group on each of Ar and Ar'; however, there should be no more than two sulfonic acid groups on the compound. The X linker is attached to the Ar and Ar' groups by amide bonds or, in the case of certain linkers within the scope of this invention, by amide analogs such as vinylogous amide and thiourea bonds. A particularly preferred linker is the urea linker (--N(CO)N--). Other examples of suitable linkers include but are not limited to: --C(CS)C-- (thiourea); --N(CO)(CO)N-- (oxalyl); --N(CO)C(CO)N-- (malonyl); --N(CO)O-- (carbamate); and --N(CO)CH₂ CH₂ (CO)N-- (succinyl), aryls or heteroaryls, squarates, and cage structures. For example, where X includes an aromatic ring, then some suitable moieties include ##STR9##

Other pyridine dicarboxylic acids may be used in preparing linkers, as can a wide variety of other aryls, heteroaryls, cage structures, and squarates, all of which are substantially rigid.

Generally, preferred compounds of the present invention are of the formula: ##STR10## wherein R₁ and R₂ individually is selected from a group consisting of substituted aryl (C₆ -C₁₂), unsubstituted aryl (C₆ -C₁₂), substituted heteroaryl (C₁ -C₁₂) and unsubstituted heteroaryl (C₁ -C₁₂), which are bound via an azo or amide group, provided that neither R₁ nor R₂ contains a sulfonic acid group, Y and Y' each is an anionic moiety, such as sulfonic, carboxylic and tetrazol, or one readily converted to anionic such as sulfonic acid ester and sulfonic acid thioester, and X is a linker as above described, which is bonded through amide or amide analogous bonds by a "J" or a "K" position link. "P" is one or more counterions, such as protons, alkali, metal, or alkaline earth cations.

Synthesis of compounds having such linkages as herein described are well established in the art, and any standard techniques described in the literature may be used, such as those outlined by Jerry March, Advanced Organic Chemistry, 4th Ed., John Wiley & Sons (1992), which is incorporated herein in its entirety by reference. For example, where X is an urea linker, one series of derivatives can be prepared by reacting 7-amino-4-hydroxynaphthalene-2-sulfonic acid (herein referred to as "J acid" (6)) with p-nitrophenylchloroformate. As shown by scheme 1, an activated intermediate is formed which is then reacted with the desired functionalized amine to form the urea product (5). ##STR11##

Another strategy involves reacting an isocyanate with J-acid. Scheme 2 illustrates this protocol. ##STR12## So that analogs may be quickly synthesized, synthetic strategies focused on using commercially available starting materials where possible. For example, many symmetric urea analogs of carbonyl-J have been synthesized using commercially available materials.

Synthetic strategies for making calcomine orange analogs are also straightforward. As seen from the structures, calcomine orange contains carbonyl-J as its core structure with additional phenyl groups linked by azo bridges. Taking advantage of the azo linkages, one strategy for making amine or amide analogs is outlined in scheme 3. ##STR13##

Another strategy is outlined in scheme 4 which takes advantage of the hydroxyl functionality directing the azo coupling to a position on a naphthalene ring. The coupling is performed by reaction of an aryl diazonium salt (which can be prepared from a wide variety of aromatic and heteroaromatic amines) with a suitably reactive aromatic receptor (i.e. carbonyl-J, J-acid). ##STR14## Although particular synthetic strategies have been outlined herein, it is to be understood that compounds of the present invention may be synthesized by any method known in the art.

Two examples of particularly preferred embodiments of the invention are: ##STR15##

The IC₅₀ for Compound 5 has been tested as 200 nM and that of Compound 159 at 220 nM. In cell-based anti-HIV (XTT) assays, Compound 5 was confirmed active.

In addition to being multienzyme inhibitors, the compounds of the present invention are remarkable in at least two other respects. First, the inventive compounds do not appear to be toxic to cells in the concentration ranges contemplated in the present invention. For example, as measured by growth curves and trypan blue exclusion of 293T cells, Compound 5 was not toxic even at concentrations greater than ten times its IC₅₀ against HIV reverse transcriptase (IC₅₀ =200 nM.

Second, the inventive compounds appear to be equally effective against mutant strains of HIV reverse transcriptase commonly found in patients who have developed resistance to current reverse transcriptase inhibitors. For example, mutant reverse transcriptase of highly resistant viruses revealed at least one the following amino acid changes: D67N, K70R, T215F/Y, K219Q, and M41L. When carbonyl-J (Compound 1) was tested against a mutant reverse transcriptase containing all of the above mutations (M41L/D67N/K70R/T215Y/K219Q), virtually no difference in inhibition was found with respect to the wild type enzyme. As a result, neither toxicity nor viral resistance appears to be a significant problem with the therapeutic use of the inventive compounds.

As stated previously, the compounds of the present invention may be used to inhibit or reduce the activities of HIV reverse transcriptase and/or HIV integrase. Methods for inhibiting these critical enzymes generally comprise administering an effective amount of at least one of the inventive compounds. As used herein, the term "effective amount" means an amount of an inventive compound which is capable of inhibiting or reducing the activity of HIV reverse transcriptase from copying single stranded RNA into double stranded DNA. However, because the compounds of the present invention are generally dual enzyme inhibitors, the term "effective amount" can also mean an amount of the inventive compound which is capable of inhibiting or reducing the activity of HIV integrase from either 3' processing or mediating DNA strand transfer or both.

Because both reverse transcriptase and integrase are necessary for replication, the compounds of the present invention may be used to inhibit, reduce, and prevent viral replication. Thus, methods for reducing or inhibiting viral replication comprise contacting an infected cell with an effective amount of one or more inventive compounds. Similarly, methods for reducing or inhibiting or preventing viral infectivity also comprise administering an infected mammal or a human patient with a suitable form of one or more of the inventive compounds.

The specific amount of an administered compound of course will depend on a number of inter-related factors including but not limited to the form of the compound, potency, mode of administration, bioavailability, age, sex and condition of the patient, all of which can be determined and assessed by one skilled in the art. For example, the potency of an individual compound may be quantified directly using enzymatic measurements, cell culture assays, or viral blood counts, or indirectly by monitoring patient progress.

Although the values may be outside of these ranges, typically, the amount or dosage per mammal or patient body weight can vary from about 0.001 mg/kg to about 150 mg/kg, and preferably between about 0.1 mg/kg and about 50 mg/kg, in one or more daily dose administrations during the course of treatment. For intravenous injection, the dose may be about 0.1 to about 30 mg/kg/day, preferably about 0.5 to about 10 mg/kg/day. If applied topically as a liquid, ointment, or cream, the compound may be present in an amount of about 0.1 to about 50 mg/ml, preferably about 0.5 to 30 mg/ml of the composition.

Another aspect of the present invention is a pharmaceutically acceptable therapeutic composition comprising one or more inventive compounds. As with dosage, the identity and the number of inventive compounds will depend on the particular circumstances. An illustrative example may include two inventive compounds where one corresponds to the most potent reverse transcriptase inhibitor and the other corresponds to the most potent integrase inhibitor. Other factors dictating the identities of the inventive compounds include but are not limited to the mode of administration, solubility (if an aqueous composition), bioavailability, therapeutic index, and half-life. In any event, although the value may be outside of this range, the total amount of the inventive compound generally is between about 1 percent and about 90 percent by weight of the formulation.

The inventive composition may further include a pharmaceutically acceptable carrier. The term "pharmaceutically acceptable" refers to materials that are compatible with the other ingredients and are not deleterious to the recipient thereof. Examples of suitable pharmaceutically acceptable carriers include, but are not limited to, buffered saline, glycols, glycerols, vegetable oils, and organic esters, and may be present in an amount between about 0.1 percent and about 90 percent by weight, and more preferably between about 20 percent and about 60 percent by weight of the formulation.

Other optional ingredients include property enhancing agents including but not limiting to stabilizers, absorption modifying agents, wetting agents, emulsifying agents, dispersing agents, biocides, preservatives, and flavoring agents, all of which are well known in the pharmaceutical art. Such property enhancing agents may be present in an amount between about zero and about 40 percent by weight, and more preferably between about 0.01 and about 20 percent by weight of the composition.

Moreover, depending on the specific circumstances, the inventive compositions may further include drug delivery vehicles such as liposomes, microspheres, or other polymer matrices. A representative publication detailing the current art is Liposome Technology, published by CRC Press in 1993, which is incorporated herein by reference.

The pharmaceutical compositions of the present invention may be in any acceptable form such as a solution, emulsion, suspension, lotion, ointment, cream, granule, powder, tablet, capsule, sachet, lozenge, ampule, or suppository, and may be administered by any method known in the art including but not limited to parenterally, intramuscularly, subcutaneously, intravenously, transdermally, orally, or topically.

Because the inventive compounds are both reverse transcriptase and integrase inhibitors that appear to be relatively unaffected by mutant virus strains, the pharmaceutical compositions of the present invention are particularly suited for combination therapy either alone or with other known antiviral agents. For example, the inventive pharmaceutical compositions either may include (or used in conjunction with) any combination of antiviral compounds. Examples include, but are not limited to, other reverse transcriptase inhibitors such as AZT, ddC, DDI, TIBO derivatives, tricyclic diazepinones, and other inhibitors of HIV enzymes such as integrase and protease. The dosages of current antiviral compounds used in the treatment of HIV infection are known in the art.

In addition, the compounds of the present invention are believed therapeutically useful in other disease states that involve retroviral replication, which are apparent to one of ordinary skill in the art upon reading this specification in light of other available knowledge. Insofar as that is the case, the treatment of various retroviral mediated disease states is meant to be encompassed herein.

Structures of representative, novel compounds of the present invention include but are not limited to those illustrated in Table 1. It is to be understood that any of the disclosed linkers, such as thiourea, oxalyl, malonyl, carbamate, and succinyl linkers, may be substituted in these illustrative structures.

Functional groups of the inventive compounds may be interchangeably illustrated in a generalized form or in a particularized form or as a salt thereof. However, all readily converted forms of the inventive compounds, whether illustrated in the tables or not, are within the scope of the present invention. For example, the sulfonic acid functionality, when present as the anionic substitutent Y and Y', of the inventive compounds are illustrated interchangeably in a generalized form ("SO₃ X" referring to ionized, unionized or a salt form thereof), or in a particularized form (e.g., ionized (SO₃ ⁻); un-ionized (SO₃ H); or as a sodium salt thereof (SO₃ ⁻ Na⁺)). Additionally, where a group is written in the center of an aromatic ring, this indicates that the group is attached to all unsubstituted positions of the ring. For example, in Compound 98, fluorene is attached at all positions except ring position 1 (attachment site to rest of molecule) and ring position 4 (carboxyl substituent).

                                      TABLE 1                                      __________________________________________________________________________     NOVEL COMPOUNDS                                                                __________________________________________________________________________                                                                   #STR16##                                                                      5                    -                                                                                                                                          6 R17##            -                                                                                                                                          7 R18##            -                                                                                                                                          8 R19##            -                                                                                                                                          9 R20##            -                                                                                                                                          10                                                                          21##      -                                                                       11                                                                          22##      -                                                                       12                                                                          23##      -                                                                       13                                                                          24##      -                                                                       14                                                                          25##      -                                                                       15                                                                          26##      -                                                                       16                                                                          27##      -                                                                       17                                                                          28##      -                                                                       19                                                                          29##      -                                                                       20                                                                          30##      -                                                                       21                                                                          31##      -                                                                       22                                                                          32##      -                                                                       23                                                                          33##      -                                                                       24                                                                          34##      -                                                                       25                                                                          35##      -                                                                       26                                                                          36##      -                                                                       27                                                                          37##      -                                                                       28                                                                          38##      -                                                                       29                                                                          39##      -                                                                       30                                                                          40##      -                                                                       31                                                                          41##      -                                                                       32                                                                          42##      -                                                                       33                                                                          43##      -                                                                       35                                                                          44##      -                                                                       36                                                                          45##      -                                                                       37                                                                          46##      -                                                                       38                                                                          47##      -                                                                       39                                                                          48##      -                                                                       40                                                                          49##      -                                                                       41                                                                          50##      -                                                                       42                                                                          51##      -                                                                       43                                                                          52##      -                                                                       44                                                                          53##      -                                                                       45                                                                          54##      -                                                                       46                                                                          55##      -                                                                       47                                                                          56##      -                                                                       48                                                                          57##      -                                                                       49                                                                          58##      -                                                                       50                                                                          59##      -                                                                       51                                                                          60##      -                                                                       52                                                                          61##      -                                                                       53                                                                          62##      -                                                                       54                                                                          63##      -                                                                       55                                                                          64##      -                                                                       56                                                                          65##      -                                                                       57                                                                          66##      -                                                                       58                                                                          67##      -                                                                       59                                                                          68##      -                                                                       60                                                                          69##      -                                                                       61                                                                          70##      -                                                                       62                                                                          71##      -                                                                       63                                                                          72##      -                                                                       64                                                                          73##      -                                                                       65                                                                          74##      -                                                                       66                                                                          75##      -                                                                       67                                                                          76##      -                                                                       68                                                                          77##      -                                                                       69                                                                          78##      -                                                                       70                                                                          79##      -                                                                       71                                                                          80##      -                                                                       72                                                                          81##      -                                                                       73                                                                          82##      -                                                                       74                                                                          83##      -                                                                       75                                                                          84##      -                                                                       76                                                                          85##      -                                                                       77                                                                          86##      -                                                                       78                                                                          87##      -                                                                       79                                                                          88##      -                                                                       80                                                                          89##      -                                                                       81                                                                          90##      -                                                                       82                                                                          91##      -                                                                       83                                                                          92##      -                                                                       84                                                                          93##      -                                                                       85                                                                          94##      -                                                                       86                                                                          95##      -                                                                       87                                                                          96##      -                                                                       88                                                                          97##      -                                                                       89                                                                          98##      -                                                                       90                                                                          99##      -                                                                       91                                                                          100##     -                                                                       92                                                                          101##     -                                                                       93                                                                          102##     -                                                                       94                                                                          103##     -                                                                       95                                                                          104##     -                                                                       96                                                                          105##     -                                                                       97                                                                          106##     -                                                                       98                                                                          107##     -                                                                       99                                                                          108##     -                                                                      100                                                                          109##     -                                                                      101                                                                          110##     -                                                                      102                                                                          111##     -                                                                      103                                                                          112##     -                                                                      104                                                                          113##     -                                                                      105                                                                          114##     -                                                                      106                                                                          115##     -                                                                      107                                                                          116##     -                                                                      108                                                                          117##     -                                                                      109                                                                          118##     -                                                                      110                                                                          119##     -                                                                      111                                                                          120##     -                                                                      112                                                                          121##     -                                                                      113                                                                          122##     -                                                                      114                                                                          123##     -                                                                      115                                                                          124##     -                                                                      116                                                                          125##     -                                                                      117                                                                          126##     -                                                                      118                                                                          127##     -                                                                      119                                                                          128##     -                                                                      120                                                                          129##     -                                                                      121                                                                          130##     -                                                                      122                                                                          131##     -                                                                      123                                                                          132##     -                                                                      124                                                                          133##     -                                                                      125                                                                          134##     -                                                                      126                                                                          135##     -                                                                      127                                                                          136##     -                                                                      128                                                                          137##     -                                                                      129                                                                          138##     -                                                                      130                                                                          139##     -                                                                      131                                                                          140##     -                                                                      132                                                                          141##     -                                                                      133                                                                          142##     -                                                                      134                                                                          143##     -                                                                      135                                                                          144##     -                                                                      136                                                                          145##     -                                                                      137                                                                          146##     -                                                                      138                                                                          147##     -                                                                      139                                                                          148##     -                                                                      140                                                                          149##     -                                                                      141                                                                          150##     -                                                                      142                                                                          151##     -                                                                      143                                                                          152##     -                                                                      144                                                                          153##     -                                                                      145                                                                          154##     -                                                                      146                                                                          155##     -                                                                      147                                                                          156##     -                                                                      148                                                                          157##     -                                                                      149                                                                          158##     -                                                                      150                                                                          159##     -                                                                      151                                                                          160##     -                                                                      152                                                                          161##     -                                                                      153                                                                          162##     -                                                                      154                                                                          163##     -                                                                      155                                                                          164##     -                                                                      156                                                                          165##     -                                                                      157                                                                          166##     -                                                                      158                                                                          167##     -                                                                      159                                                                          168##     -                                                                      160                                                                          169##     -                                                                      161                                                                          170##     -                                                                      162                                                                          171##     -                                                                      163                                                                          172##     -                                                                      164                                                                          173##     -                                                                      165                                                                          174##     -                                                                      166                                                                          175##     -                                                                      167                                                                          176##     -                                                                      168                                                                          177##     -                                                                      169                                                                          178##     -                                                                      170                                                                          179##     -                                                                      171                                                                          180##     - 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                                                                     186                                                                          195##     -                                                                      187                                                                          196##     -                                                                      188                                                                          197##     -                                                                      189                                                                          198##     -                                                                      190                                                                          199##     -                                                                      191                                                                          200##     -                                                                      192                                                                          201##     -                                                                      193                                                                          202##     -                                                                      194                                                                          203##     -                                                                      195                                                                          204##     -                                                                      196                                                                          205##     -                                                                      197                                                                          206##     -                                                                      198                                                                          207##     -                                                                      199R208##        __________________________________________________________________________

Aspects of the invention will now be illustrated by the following examples. It will be understood that these examples are intended to illustrate, and not limit, the present invention.

EXAMPLE 1

General Procedure for Symmetric Ureas

A solution of amine (2 equivalents) is dissolved in CH₂ Cl₂ and treated with CDI in CH₂ Cl₂ (1 equivalent), and then shaken for 12-24 hours. If substantial amounts of the product precipitates, it can be removed at this point. If no precipitate is formed, then the reaction is partitioned between water and CH₂ Cl₂. The organic layer is dried over Na₂ SO₄ and evaporated to give the crude urea which, if possible, is recrystallized.

General Procedure for Hetero Ureas

A solution of 4-nitrophenoxychloroformate (1 equivalent) is dissolved in CH₂ Cl₂ and THF at a concentration such that at -78° C. no precipitate forms. A solution of the least nucleophilic amine and TEA or pyridine (1 equivalent each) in CH₂ Cl₂ is slowly added at -78° C., stirred for 15 minutes at -78° C. and then warmed slowly to room temperature. After stirring for 45 minutes at room temperature, the second amine is added (1 equivalent) and the resulting solution is stirred for 1 to 3 days depending on the reactivity of the amine used.

The product is extracted with Na₂ CO₃ solution (5-25% of saturation appears to work best) until the yellow color of the reaction mixture has been eliminated (approximately between 2 and 4 extractions). Sometimes a 20% H₂ SO₄ is used to remove excess amines prior to the carbonate extractions. However, this step is omitted if no severe amine contamination is present as determined by thin layer chromatography ("TLC"), or if the final product contains a basic site. The organic extracts are dried over Na₂ SO₄ and evaporated. If possible, the crude products are recrystallized.

EXAMPLE 2

Experimental Protocol for Analogs of Calcomine Orange

Procedures were performed in batches of 12 reactions (the limit of the centrifuge rotor) using 50 ml disposable centrifuge cones. Because some of the diazonium salts formed may be unstable, it is best to use them immediately after their formation.

A sample of the desired aniline functionality (1 eq.) is suspended or dissolved in 1 ml of water and 0.25 ml of 20 percent sulfuric acid. A solution of NaNO₂ (1 eq.) is added and the resulting solution is mixed for about 1-5 minutes until 95% or more material dissolves. At this point, the solution usually turns clear yellow.

The solution is then added to 5 ml of water and saturated carbonate solution is added until the pH of the mixture reaches about 9. The compound to be derivatized (J-acid (1 eq.) or carbonyl J or an analog thereof (1/2 eq.)) is then added, generally resulting in a deeply colored solution. The mixture is stirred at room temperature for approximately 2 hours during which water may be additionally added to aid in the mixing process. The mixture is then acidified with a 20 percent solution of sulfuric acid, diluted with water to a total volume of 35 ml, and centrifuged at 5000 G for about 30 minutes.

After centrifugation, the supernatant is removed and the precipitate is washed usually with 25 ml H₂ O, then 5 to 15 ml of ethanol (or methanol) depending on the amount of precipitate and solubility. The resulting paste is dried overnight under a vacuum which yields the desired compound (usually black, flaky solid). The compound is then usually characterized using one dimensional NMR spectroscopy.

Oxallyl Bis(J-acid)diamide Diimidazole Salt

A mixture of oxallyl diimidazole (1.98 g), J-acid (5.00 g, dried on pump overnight), and imidazole (1.60 g, recrystallized from benzene) was diluted with DMF (20 ml, dry) and allowed to stir. After a few hours the reaction became cloudy and remained cloudy for the duration of the reaction. After 4 days the reaction mixture was centrifuged, and the pelleted material washed with ethanol (4×10-15 ml) until the liquid layer was only lightly colored. The material was dried in vacuum to yield 2.67 g of an off white powder.

General procedure for Oxallyl Bis(J-acid)diamide Azo Derivatives

A sample of an aniline (typical example is p-aminohydrocinnamic acid, 2 eq) is suspended or dissolved in 0.5 ml water and 0.25 ml of 20% H₂ SO₄ is added. Separately oxallyl bis(J-acid)diamide diimidazole salt (1 eq) is diluted with 2 ml water and 0.4 ml saturated Na₂ CO₃ solution. Although this mixture does not initially dissolve, the mixture is heated until dissolution occurs. If undissolved material is used, the reaction fails almost completely. A solution of NaNO₂ (2 eq) in 0.5 ml water is added to the starting aniline solution, and the resulting solution mixed for about 2-3 minutes (usually the solution turns clear and yellow). The solution is then added to 5 ml water and saturated carbonate solution is added until the pH of the mixture reaches about 9. The warm (may be hot), fully dissolved, oxallyl bis(J-acid)diamide diimidazole salt solution is then added, which generally results in a deeply-colored solution. The mixture is allowed to stir at room temperature for 2 hours (additional water may be added as necessary), then acidified with 20% H₂ SO₄ (pH-1), diluted with water to a total volume of 35 ml, and centrifuged (5000 g, 30 min). The precipitate is washed with water (amount depending on the amount of precipitate, maximum of 25 ml), then with ethanol 5-15 ml (depending on its amount and solubility). The resulting paste is dried overnight under vacuum to yield the desired compound, generally as a black, flaky solid. Characterization is performed by ¹ H NMR.

EXAMPLE 3

Preparation of Compound 160:

To 1.20 g imidazole in 20 ml CH₂ Cl₂ was added a slurry of tera phtholyl dichloride (885 mg) in 10 ml CH₂ Cl₂, and the reaction allowed to stir at room temperature for 15 hours. The entire mixture is evaporated in vacuum and a solution of 10 ml dry DMF, J-acid (1.90 g) and imidazole (0.88 g) was added. After stirring 23 hours at room temperature, the mixture is evaporated to a tar under vacuum and 60 ml of water was added. The initial tar dissolves then precipitates a gray powder which is isolated by centrifigation followed by washing with 2×10 ml portions of water. The product was pumped dry to yield 0.455 g of the desired product.

Preparation of Compound 161:

59 gm of 4-aminocinniaminic acid hydrochloride salt was slurred in 0.5 ml of water and 0.25 ml of 20% H₂ SO₄ was added followed by a solution of 19.5 mg NaNO₂ in 0.5 ml H₂ O. The reaction was mixed with a pipette until 95+% of the precipitate dissolved and was then added to 3 ml H₂ O. The solution was bacisified with Na₂ CO₃ saturated solution to pH of about 9 was reached. A solution of Compound 60 (99 mg) fully dissolved in 4 ml warm water and 0.4 ml Na₂ CO₃ solution was added and the reaction mixture immediately turned dark purple/red. The resulting solution was allowed to stir at room temperature for 2 hours after which time it was diluted to half concentration with water and acidified with 20% H₂ SO₄ to a pH of approximately 0. The resulting slurry was again diluted with water to 1/2 concentration and the precipitate isolated by centrifugation. The precipitate was washed with water (2×15 ml) and ethanol 10 ml) then dried under vacuum overnight to yield 119 mg of the desired compound.

Preparation of the Compound Series 162-173:

The following general procedure was used to run azo addition reactions in a 12 reaction format. Diazonium salts were generated from the appropriate aniline by suspending the aniline (1 equivalent) in 0.5 ml H₂ O and 0.1 ml 20% H₂ SO₄, followed by the addition of 1 equivalent of NaNO₂ in 0.5 ml H₂ O. The resulting mixture was mixed with a pipette until 95%+ of the material had dissolved, but never less than 30 seconds and no more than five minutes, and was then added to 5 ml H₂ O in a 50 ml centrifuge cone. The mixture was bacisified with Na₂ CO₃ saturated solution to a pH greater than 9 (about 1 ml was required) 3 ml of Compound 60 solution (0.5 eq) was added (stock solution made by mixing 34 ml H₂ O, 2 ml Na₂ CO₃, and 455 mg Compound 60) the reaction mixture usually turned dark red in color and was set to stir while the next reaction was performed. After stirring the reactions for 1.75 hours the reactions were all acidified with 20% H₂ SO₄ (to pH≦1) and the materials were centrifuged. The pelleted material was retained and washed with water (2×7.5 ml) and ethanol (2 ml) then dried in vacuum overnight to yield the desired products. Note that products which did not readily precipitate on acidification could some times be salvaged by addition of saturated NaCl solution, followed by only the ethanol wash. The identity of products was confirmed by H¹ NMR purity varied from 95+% to less than 50%. Compounds deemed clean enough for further work was tested for biological activity.

Preparation of Compound 184:

A mixture of dimethyl squareate (233 mg), J acid (774 mg), imidazole (600 mg) and dry DMF (5 ml) was heated overnight at 100° C. (total 22 hours). The reaction mixture was diluted with 25 ml ethanol, producing a precipitate which was isolated by centrifugation, washed with ethanol (30 ml), ethyl acetate (2×40 ml) and dried in vacuum to yield. 7477 g of the desired product.

Preparation of Compound 185:

47.5 mg of 4-aminocinniaminic acid hydrochloride salt was slurred in 0.5 ml of water and 0.25 ml of 20% H₂ SO₄ was added followed by a solution of 14.2 mg NaNO₂ in 0.5 ml H₂ O. The reaction was mixed with a pipette until 95+% of the precipitate dissolved and was then added to 3 ml H₂ O. The solution was bacisified with Na₂ CO₃ saturated solution to pH of about 9 was reached. A solution of Compound 184 (50.6 mg) fully dissolved in 2 ml warm water with enough Na₂ CO₃ added to effect solution, was added and the reaction mixture which immediately turned dark purple/red. The resulting solution was allowed to stir at room temperature for 3 hours after which time it was diluted to half concentration with water and acidified with 20% H₂ SO₄ to a pH less than 1. The resulting slurry was centrifuged and the precipitate was washed with water (2×20 ml) ethanol (2×5 ml) and ethyl acetate (2×5 ml) then dried under vacuum overnight to yield 62.5 mg of the desired compound.

Preparation of the Compound Series 186-197:

The following general procedure was used to run azo addition reactions in a 12 reaction format. Diazonium salts were generated from the appropriate aniline by suspending the aniline (1 equivalent) in 0.5 ml H₂ O and 0.25 ml 20% H₂ SO₄, followed by the addition of 1 equivalent of NaNO₂ in 0.5 ml H₂ O. The resulting mixture was mixed with a pipette until 95%+ of the material had dissolved, but never less than 30 seconds and no more than five minutes, and was then added to 5 ml H₂ O in a 50 ml centrifuge cone. The mixture was bacisified with 2 ml Na₂ CO₃ saturated solution 3 ml of Compound 184 (0.5 eq ) was added (stock solution made by mixing 36 ml H₂ O, 623 mg Compound 184, and sufficient Na₂ CO₃ to effect solution) the reaction mixture usually turned dark red in color and was set to stir while the next reaction was performed. After stirring the reactions for 2.5 hours the reactions were all acidified with 20% H₂ SO₄ (to pH≦1, approx. 1 ml), diluted with water to 25 ml total volume and centrifuged. The pelleted material was retained and washed with water (10 ml) and ethanol (7.5 ml) and the remaining precipitate was dried in vacuum. The identity of products was confirmed by H¹ NMR purity varied from 95+% to less than 50%. Compounds deemed clean enough for further work were tested for biological activity.

Preparation of Compound 117:

To 1.01 g 2,6-pyridine dicarboxcylic acid and 2.10 g carbonyl diimidazole was added 20 ml dry DMF. The reaction was allowed to stir at room temperature with the evolution of CO₂ for 22 hours. J acid was then added (2.80 g, dried under vacuum overnight prior to use) and the mixture allowed to stir an additional 24 hours. The mixture was diluted with 100 ml ethanol then with 150 ml ethyl acetate. The resulting initial tarry precipitate was discarded and the mixture was further diluted to 1000 ml volume with ethyl acetate. The resulting precipitate was isolated by centrifugation, washed with ethylacetate and dried in vacuum to yield 1.062 g of the desired product.

Preparation of Compound 118:

39.5 of 4-aminobenzoic acid was slurred in 0.5 ml of water and 0.25 ml of 20% H₂ SO₄ was added followed by a solution of 18.6 mg NaNO₂ in 0.5 ml H₂ O. The reaction was mixed with a pipette until 95+% of the precipitate dissolved and was then added to 3 ml H₂ O. The solution was bacisified with Na₂ CO₃ saturated solution to pH of about 9 was reached. A solution of Compound 117 (100 mg) fully dissolve din 2 ml warm water and 0.5 ml Na₂ CO₃ solution, was added and the reaction mixture which immediately turned dark purple/red. The resulting solution was allowed to stir at room temperature for 2.5 hours after which time it was acidified with 20% H₂ SO₄ to a pH of approximately 0 and diluted with 3 ml water. The precipitate was isolated by centrifugation washed with water (10 ml then 2×5 ml) and methanol (5 ml) and ethyl acetate (5 ml) then dried under vacuum over night to yield 92.6 mg of the desired compound.

Preparation of the Compound Series 119-130:

The following general procedure was used to run azo addition reactions in a 12 reaction format. Diazonium salts were generated from the appropriate aniline by suspending the aniline (1 equivalent) in 1.0 ml H₂ O and 0.25 ml 20% H₂ SO₄, followed by the addition of 1 equivalent of NaNO₂ in 0.5 ml H₂ O. The resulting mixture was mixed with a pipette until 95%+ of the material had dissolved, but never less than 30 seconds and no more than five minutes, and was then added to 5 ml H₂ O in a 50 ml centrifuge cone. The mixture was bacisified with 2 ml Na₂ CO₃ saturated solution, 2 ml of Compound 117 solution (0.5 eq) was added (stock solution made by mixing 18 ml H₂ O, 6 ml Na₂ CO₃ and Compound 117 900 mg) the reaction mixture usually turned dark red in color and was set to stir while the next reaction was performed. After stirring the reactions for 2.25 hours the reactions were all acidified with 20% H₂ SO₄ (2 ml), diluted to 35 ml total volume and the materials were centrifuged. The pelleted material was retained and washed with water (15 ml) and ethanol (15 ml) then dried in vacuum overnight to yield the desired products. Note that products which were excessively soluble could some times be salvaged by addition of ethyl acetate/chloroform. The identity of products was confirmed by H¹ NMR purity varied from 95+% to less than 50%. Compound deemed clean enough for further work were tested for biological activity.

Preparation of Compound 131:

To 1.35 g chelidonic acid and 2.60 g carbonyl di imidazole was added 10 ml dry DMF. The reaction was allowed to stir at room temperature with the evolution of CO₂ for 19 hours. J acid was then added (3:33 g, dried under vacuum overnight prior to use) and the mixture allowed to stir an additional 24 hours. The mixture was diluted with 100 ml ethanol and the resulting precipitate was isolated by centrifugation, washed with ethanol (3×20 ml) and ethylacetate (2×20 ml) and dried in vacuum to yield 3.006 g of the desired product as a yellow powder.

Preparation of Compound 132:

36 of 4 aminobenzoic acid was slurred in 0.6 ml of water and 0.25 ml of 20% H₂ SO₄ was added followed by a solution of 18 mg NaNO₂ in 0.5 ml H₂ O. The reaction was mixed with a pipette until 95+% of the precipitate dissolved and was then added to 3 ml H₂ O. The solution was bacisified with Na₂ CO₃ saturated solution to pH of about 9 was reached. A solution of Compound 131 (88.6 mg) fully dissolved in 2 ml warm water and 0.5 ml Na₂ CO₃ solution, was added and the reaction mixture which immediately turned dark purple/red. The resulting solution was allowed to stir at room temperature for 3 hours after which time it was acidified with 20% H₂ SO₄ to a pH of approximately 0 and diluted with 5 ml water. The precipitate was isolated by centrifugation washed with water (2×5 ml) and ethanol (5 ml) then dried under vacuum overnight to yield 85.6 mg of the desired compound.

Preparation of the Compound Series 133-144:

The following general procedure was used to run azo addition reactions in a 12 reaction format. Diazonium salts were generated from the appropriate aniline by suspending the aniline (1 equivalent) in 0.5 ml H₂ O and 0.25 ml 20% H₂ SO₄, followed by the addition of 1 equivalent of NaNO₂ in 0.5 ml H₂ O. The resulting mixture was mixed with a pipette until 95%+ of the material had dissolved, but never less than 30 seconds and no more than five minutes, and was then added to 5 ml H₂ O in a 50 ml centrifuge cone. The mixture was bacisified with 2 ml Na₂ CO₃ saturated solution, 2 ml of Compound 131 solution (0.5 eq) was added (stock solution made by mixing 18 ml H₂ O, 6 ml Na₂ CO₃ and Compound 131 1.20 g) the reaction mixture usually turned dark red in color and was set to stir while the next reaction was performed. After stirring the reactions for 2 hours the reactions were all acidified with 20% H₂ SO₄ (2 ml), diluted to 25 ml total volume and the materials were centrifuged. The pelleted material was retained and washed with water (15 ml) and ethanol (15 ml) then dried in vacuum overnight to yield the desired products. Note that products which were excessively soluble could some times be salvaged by addition of further acid and skipping the water wash. The identity of products was confirmed by H¹ NMR purity varied from 95+% to less than 50%. Compounds deemed clean enough for further work were tested for biological activity.

Preparation of Compound 145:

To 1.01 g chelidamic acid (hydrate, pumped overnight to dry) and 1.92 g carbonyl diimidazole was added 10 ml dry DMF. The reaction was allowed to stir at room temperature with the evolution of CO₂ overnight. J acid was then added (2.32 g, dried under vacuum overnight prior to use) and the mixture allowed to stir an additional 5 days. The reaction mixture was centrifuged and the initial precipitate discarded. The remaining liquid was added to 100 ml ethanol and the mixture let stand 30 minutes. The resulting precipitate was isolated by centrifugation, washed with ethanol (3×10 ml) and ethylacetate (2×10 ml) and dried in vacuum to yield 1.56 g of the desired product as a gray/brown powder.

Preparation of Compound 146:

37.5 of 4 aminobenzoic acid was slurred in 0.5 ml of water and 0.25 ml of 20% H₂ SO₄ was added followed by a solution of 18.7 mg NaNO₂ in 0.5 ml H₂ O. The reaction was mixed with a pipette until 95+% of the precipitate dissolved and was then added to 3 ml H₂ O. The solution was bacisified with Na₂ CO₃ saturated solution to pH of about 9 was reached. A solution of Compound 145 (99.1 mg) fully dissolved in 2 ml warm water and 0.5 ml Na₂ CO₃ solution, was added and the reaction mixture which immediately turned dark purple/red. The resulting solution was allowed to stir at room temperature for 4.5 hours after which time it was acidified with 20% H₂ SO₄ to a pH of approximately 0 and diluted to half concentration with water. The precipitate was isolated by centrifugation washed with water (2×20 ml) and ethanol (20 ml, then 10 ml) and ethyl acetate (2×10 ml) then dried under vacuum overnight to yield 75.7 mg of the desired compound.

Preparation of the Compound Series 147-158:

The following general procedure was used to run azo addition reactions in a 12 reaction format. Diazonium slats were generated from the appropriate aniline by suspending the aniline (1 equivalent) in 0.5 ml H₂ O and 0.25 ml 20% H₂ SO₄, followed by the addition of 1 equivalent of NaNO₂ in 0.5 ml H₂ O. The resulting mixture was mixed with a pipette until 95%+ of the material had dissolved, but never less than 30 seconds and no more than five minutes, and was then added to 5 ml H₂ O in a 50 ml centrifuge cone. The mixture was bacisified with 2 ml Na₂ CO₃ saturated solution, 2 ml of J-2,6 40 h Compound 145 solution (0.5 eq) was added (stock solution made by mixing 18 ml H₂ O, 6 ml Na₂ CO₃ and Compound 145 1.20 g) the reaction mixture usually turned dark red in color and was set to stir while the next reaction was performed. After stirring the reactions for 2 hours the reactions were all acidified with 20% H₂ SO₄ (2 ml), diluted to 30 ml total volume and the materials were centrifuged. The pelleted material was retained and washed with water (15 ml) and ethanol (30 ml) then dried in vacuum overnight to yield the desired products. Note that products which were excessively soluble in ethanol could some times by salvaged by addition ethyl acetate to the ethanol wash to initiate precipitation. The identity of products was confirmed by H¹ NMR purity varied from 95+% to less than 50%. Compounds deemed clean enough for further work were tested for biological activity.

EXAMPLE 4

Reverse Transcriptase Assay

Reverse transcriptase ("RT") activity is measured using a scintillation proximity assay kit available from Amersham Life Sciences, Inc., which uses a biotin/streptavidin bead capture system. RNA-dependent polymerase activity is measured using purified RH enzyme and a synthetic 17mer/50mer RNA-DNA template-primer containing biotin at the 5' end of the DNA. The template-primer, buffer, dNTP, and inhibitor are incubated for 10 minutes at 37° C. before the RT is added. The final 100 μl reaction mixture contains: 39 nm of template primer, buffer (40 mM tris HCl at pH 8.0, 10 mM MgCl₂, 60 mM KCl, 10 mM dithiothreitol); 75 nM of each dNTP except dTTP; 25 nM dTTP and 35 nM tritium labeled d*TTP; 10 μM inhibitor; and 1.0-2.0 μg of RT. After three minute incubation, the reaction is quenched with 40 μl of 0.56M EDTA. Then 10 μl of streptavidin SPA beads (in suspension) are added and incubated at 37° C. for 10 minutes. Finally, 850 μl of a buffer containing 10 mM Tris HCl pH 7.4 and 0.15M NaCl is added. The signal is produced by biotinylated polymers incorporating d*TTP binding to the streptavidin beads which stimulate the scintillant. The amount of d*TTP incorporated in the polymer is measured with a scintillation counter.

Compounds showing good inhibition will give a low number of counts/min (cpm). This number is related to a standard, dimethyl sulfoxide, which is given an arbitrary 100% relative activity. All cpm data in a single run are given a percent of this standard.

                  TABLE 2                                                          ______________________________________                                                     % RT activity remaining at 10 μM                                  INHIBITOR (or IC.sub.50  if designated as such)                              ______________________________________                                         Compound 1  IC.sub.50  = 5 μM                                                 Compound 4 IC.sub.50  = 1.5 μM                                              Compound 5 IC.sub.50  = 200 nM                                                 Compound 6 84%                                                                 Compound 7 78%                                                                 Compound 8 83%                                                                 Compound 9 75%                                                                 Compound 10 88%                                                                Compound 11 90%                                                                Compound 12 88%                                                                Compound 13 82%                                                                Compound 14 90%                                                                Compound 15 88%                                                                Compound 16 81%                                                                Compound 17 82%                                                                Compound 19 80%                                                                Compound 20 86%                                                                Compound 21 108%                                                               Compound 22 100%                                                               Compound 23 100%                                                               Compound 24 90%                                                                Compound 25 86%                                                                Compound 26 88%                                                                Compound 27 80%                                                                Compound 28 100%                                                               Compound 29 108%                                                               Compound 30 87%                                                                Compound 31 IC.sub.50  = 390 nM                                                Compound 32 IC.sub.50  = 500 nM                                                Compound 33 IC.sub.50  = 500 nM                                                Compound 35 IC.sub.50  = 500 nM                                                Compound 36 IC.sub.50  = 500 nM                                                Compound 37 16%                                                                Compound 38 47%                                                                Compound 39 12%                                                                Compound 40 31%                                                                Compound 41 66%                                                                Compound 42 47%                                                                Compound 43 52%                                                                Compound 44 19%                                                                Compound 45   2.8%                                                             Compound 46   4.6%                                                             Compound 47  2%                                                                Compound 48 17%                                                                Compound 49  1%                                                                Compound 50   1.3%                                                             Compound 51   1.1%                                                             Compound 52   1.3%                                                             Compound 53 IC.sub.50  = 600 nM                                                Compound 54   0.6%                                                             Compound 55 24%                                                                Compound 56 27%                                                                Compound 57   0.6%                                                             Compound 58 IC.sub.50  = 800 nM                                                Compound 59   2.0%                                                             Compound 60  6%                                                                Compound 61 53%                                                                Compound 75 85%                                                                Compound 76 88%                                                                Compound 77 84%                                                                Compound 78 80%                                                                Compound 79 78%                                                                Compound 80 84%                                                                Compound 81 78%                                                                Compound 82 92%                                                                Compound 83 77%                                                                Compound 84   1.7%                                                             Compound 86 IC.sub.50  = 1.2 μM                                             Compound 118    .25%                                                           Compound 119    .29%                                                           Compound 120    .21%                                                           Compound 121    .16%                                                           Compound 123    .2%                                                            Compound 124   1.2%                                                            Compound 126    .16%                                                           Compound 127    .14%                                                           Compound 128  5%                                                               Compound 130    .35%                                                           Compound 131 48%                                                               Compound 132    .19%                                                           Compound 133    .4%                                                            Compound 134    .25%                                                           Compound 135    .16%                                                           Compound 137    .53%                                                           Compound 139    .34%                                                           Compound 143    .23%                                                           Compound 144    .26%                                                           Compound 145 47%                                                               Compound 147    .3%                                                            Compound 150    .6%                                                            Compound 151    .2%                                                            Compound 153    .15%                                                           Compound 156 15%                                                               Compound 159 IC.sub.50  = 220 nm                                               Compound 160 74%                                                               Compound 161 25%                                                               Compound 162   5.9%                                                            Compound 163    .1%                                                            Compound 164    .15%                                                           Compound 165   3.7%                                                            Compound 166    .14%                                                           Compound 167    .26%                                                           Compound 168    .50%                                                           Compound 169    .15%                                                           Compound 170    .10%                                                           Compound 171    .15%                                                           Compound 172    .08%                                                           Compound 173 27%                                                               Compound 174 28%                                                               Compound 175 62%                                                               Compound 176 60%                                                               Compound 177    .17%                                                           Compound 178 91%                                                               Compound 179   7.5%                                                            Compound 180 45%                                                               Compound 181 43%                                                               Compound 182 35%                                                               Compound 183 36%                                                               Compound 184  IC.sub.50  = 1000 nM                                             Compound 185    .6%                                                            Compound 186    .5%                                                            Compound 187    .3%                                                            Compound 188    .3%                                                            Compound 189   1.0%                                                            Compound 190    .5%                                                            Compound 191    .3%                                                            Compound 192    .3%                                                            Compound 193    .4%                                                            Compound 194 IC.sub.50  = 440 nM                                               Compound 198 37%                                                               Compound 199   1.2%                                                          ______________________________________                                    

The anti-viral evaluations branch of the National Institutes of Health also ran cell-based anti-HIV (XTT) assays and reverse transcriptase (RT) assays on a number of the novel compounds. FIG. 1 graphically illustrates the reverse transcriptase assay and FIG. 2 the primary (XTT) screen run for Compound 5, which lead to a "confirmed active" conclusion. Other novel compounds of this invention were similarly confirmed as active or moderately active by these tests. These were: 31, 32, 35, 36, 53, 54, 57, 58, 91, 99, and 103.

EXAMPLE 5

Reverse Transcriptase Mutant Assays

The mutants were constructed using BspMI cassette mutagenesis as described previously by Boyer et al. (J Virol., 66:1031-1039 and 7533-7537 (1992)), which is hereby incorporated by reference. The RT assay has also been previously described by Boyer et al. (PNAS USA, 91:4882-4886 (1994)), which is also incorporated by reference. Briefly, RNA dependent DNA polymerase activity is assayed using purified RT protein and a poly(rC).olio(dG) template-primer as the substrate. The protein (1 μg) and substrate are assayed in a total reaction volume of 100 μl containing 0.01 unites poly(rC).olio(dG), 0.02 mM dGTP, 0.002 mCi [α-³² P]dGTP, and a buffer containing 25 mM tris (pH 8.0), 75 mM KCL, 8.0 mM MgCl₂, 2.0 mM dithiothreitol, and 10 mM 3-[(3-cholamidopropyl) diethylammoniol]-1-propane-sulfonate containing acetylated bovine serum albumin at 100 μg/ml. The assay mixture is incubated for 30 minutes, and then stopped by the addition of 50 μl of a 10 mg/ml solution of sheared and denatured salmon sperm DNA followed by 3.0 ml 10 percent trichloroacetic acid. The labeled polymer is collected by suction filtration on Whatman glass GF/C and counted.

Inhibition results of mutant reverse transcriptase are presented in Table 3. As the data shows, carbonyl J (Compound 1) displays activity against non-nucleoside mutants as well as other mutants that have been shown to be problematic for most HIV-1 RT inhibitors.

                  TABLE 3                                                          ______________________________________                                         Reverse Transcriptase                                                                         % Activity Remaining Using Carbonyl J                             Mutant (Compound 1) at 10 μM and 50 μM                                 ______________________________________                                         WT             29           3                                                    L100I 11 1                                                                     K103N 32 3                                                                     V106A 33 4                                                                     Y181I 18 1                                                                     Y188L 23 2                                                                     E138K 29 4                                                                     P236L 35 4                                                                     L74V 34 6                                                                      M184V 42 5                                                                     AZT-21 33 4                                                                    {M41L/D67N/K70R/T215                                                           Y/K219Q}                                                                     ______________________________________                                    

EXAMPLE 6

Cell Culture Integrase Assay

The plasmid containing the env-deleted HIV-1 genome and the plasmid containing the chosen env gene are co-transfected into 293T cells. Viral particles released into the media are harvested and used to infect an appropriate cell line (i.e. 3T3 cells for ecotropic-MLV envelope, various murine and human cells for amphotropic-MLV env, and CD4-expressing cells for HIV-1 envelope) and selected for hygromycin resistance colonies. ("HRCs"). The number of HRCs per unit volume of stock is a direct quantification of the number of viral particles per unit volume of stock that can form a provirus. Reductions in the number of HRCs in the presence of an inhibitor indicate a block to infection somewhere between cell entry and integration. Extrachromosomal DNA harvested shortly after infection can be used to determine if there has been a block in migration of the preintegration complex ("PIC") from the cytoplasm to the nucleus. If circular DNA is not reduced relative to circular DNA generated in the absence of the inhibitor, the reductions in provirus formations are most likely due to a direct impairment of integrase activity.

EXAMPLE 7

The protocol for assaying integrase inhibitors has been previously described in Leavitt et al., J Virology, 66:2359-68 (1992), which is incorporated by reference herein. Briefly, inhibitor and 5 pmol of integrase are pre-incubated in 15 μl of reaction buffer (50 mM MOPS (3-[N-morpholino]propane-sulfonic acid), pH 7.0, 15 mM MnCl₂, and 10 mM DTT) for 5 minutes at room temperature prior to the introduction of DNA substrate which marks the start of the reaction. Once 0.5 pmol of DNA substrate is added, the reaction is allowed to continue for 20 minutes. The reaction is then stopped by the addition of 95% formamide and heating to 100° C. for 2 minutes. Potential inhibitors are screened at a single concentration, and those with inhibitory activity are then put through a dose response assay to determine the concentration at which integrase activity is decreased by 50% (IC₅₀).

                  TABLE 4                                                          ______________________________________                                                        Inhibition of 3'                                                                            Inhibition of strand                                  processing activity transfer                                                  Inhibitor (IC.sub.50) (IC.sub.50)                                            ______________________________________                                         Compound 1     2.5    μM     2.5  μM                                       Compound 4 2.0 μM 2.0 μM                                                 Compound 5 0.9 μM 1.0 μM                                                 Compound 31 0.4 μM 0.7 μM                                                Compound 32 2.0 μM 0.7 μM                                                Compound 33 0.3 μM 0.6 μM                                                Compound 34 2.0 μM 2.0 μM                                                Compound 35 0.8 μM 2.0 μM                                                Compound 36 0.8 μM 1.0 μM                                                Compound 37 >3 μM >3 μM                                                  Compound 38 >3 μM >3 μM                                                  Compound 39 2.0 μM 3.0 μM                                                Compound 40 >3 μM >3 μM                                                  Compound 41 >20 μM >20 μM                                                Compound 42 >3 μM >3 μM                                                  Compound 43 >20 μM >20 μM                                                Compound 45 >3 μM >3 μM                                                  Compound 46 >3 μM >3 μM                                                  Compound 47 >3 μM >3 μM                                                  Compound 48 >3 μM >3 μM                                                  Compound 49 2.0 μM 1.0 μM                                                Compound 50 2.0 μM 2.0 μM                                                Compound 51 0.5 μM 0.9 μM                                                Compound 52 0.2 μM 0.5 μM                                                Compound 53 0.5 μM 2.0 μM                                                Compound 54 4.0 μM 2.0 μM                                                Compound 55 >3 μM >3 μM                                                  Compound 56 >3 μM >3 μM                                                  Compound 57 0.6 μM 0.9 μM                                                Compound 58 0.2 μM 0.6 μM                                                Compound 59 2.0 μM 1.0 μM                                                Compound 60 0.8 μM 2.0 μM                                                Compound 61 >3 μM >3 μM                                                  Compound 62 0.4 μM 0.5 μM                                                Compound 64 >3 μM >3 μM                                                  Compound 65 0.8 μM 0.5 μM                                                Compound 66 0.8 μM 0.5 μM                                                Compound 67 0.09 μM 0.25 μM                                              Compound 68 0.4 μM 0.4 μM                                                Compound 69 0.7 μM 0.9 μM                                                Compound 70 >3 μM >3 μM                                                  Compound 71 0.9 μM 1.0 μM                                                Compound 72 1.0 μM 0.5 μM                                                Compound 73 1.0 μM 0.6 μM                                                Compound 74 2.0 μM 1.5 μM                                                Compound 93 0.9 μM 0.5 μM                                                Compound 94 1.0 μM 0.4 μM                                                Compound 95 0.4 μM 0.7 μM                                                Compound 96 0.5 μM 0.4 μM                                                Compound 97 0.5 μM 1.0 μM                                                Compound 98 0.4 μM 0.2 μM                                                Compound 99   0.3 μM                                                        Compound 100 0.4 μM 0.7 μM                                               Compound 101 0.5 μM 2.0 μM                                               Compound 102 0.6 μM 0.7 μM                                               Compound 103 <1 μM <1 μM                                                 Compound 104 0.6 μM 0.4 μM                                               Compound 106 1.5 μM 0.4 μM                                               Compound 107 0.7 μM 0.5 μM                                               Compound 108 1.0 μM 0.7 μM                                               Compound 110 1.1 μM 0.4 μM                                               Compound 114 1.0 μM 0.3 μM                                             ______________________________________                                    

It is to be understood that while the invention has been described above in conjunction with preferred specific embodiments, the description and examples are intended to illustrate and not limit the scope of the invention, which is defined by the scope of the appended claims. 

What is claimed is:
 1. A method for treating a retroviral infection in a patient in need thereof comprising administering to the patient a therapeutically effective amount of a naphthol compound, or a pharmaceutically acceptable salt thereof, having the structure: ##STR209## wherein R₁ and R₂ each is selected from a group consisting of substituted aryl (C₆ -C₁₂), unsubstituted aryl (C₆ -C₁₂), substituted heteroaryl (C₂ -C₁₂) and unsubstituted heteroaryl (C₁ -C₁₂), wherein the heteroatom is nitrogen, bound via an azo or amide group, provided that neither R₁ nor R₂ contains a --SO₃ H group, Y and Y' each is selected from the group consisting of --SO₃ H, --COOH esters of --SO₃ H and --COOH, and tetrazolyl, and X is a substantially rigid linker, wherein the linker is:(a) derived from the group consisting of urea, thiourea, oxalyl, malonyl, carbamate, succinyl, and vinylogous amide; (b) an aryl or heteroaryl, where the heteroatom is nitrogen or oxygen; or (c) a squarate or a cage structure.
 2. The method as in claim 1 wherein the naphthol compound or salt thereof is administered orally, topically, or by injection.
 3. A method for treating a retroviral infection in a patient in need thereof comprising:administering to the patient a therapeutically effective amount of a napthol compound, or a pharmaceutically acceptable salt thereof, wherein the naphthol or salt administered is: ##STR210## where Y and Y' each is selected from the group consisting of sulfo, carboxyl, tetrazolyl, sulfonic acid ester, and sulfonic acid thioester, X is a substantially rigid linker wherein the linker is: (a) derived from the group consisting of urea, thiourea, oxalyl, malonyl, carbamate, succinyl, and vinylogous amide; (b) an aryl or heteroaryl, where the heteroatom is nitrogen or oxygen; or (c) a squarate or a cage structure, Z is an azo or amide linkage, and one or both of R₃ and R₄ is a carboxyl, a triazolyl, or a tetrazolyl group, with the proviso that when sulfo groups are present there are no more than two.
 4. A method for treating a retroviral infection in a patient in need thereof comprising:administering to the patient a therapeutically effective amount of a napthol compound, or a pharmaceutically acceptable salt thereof, wherein the naphthol or salt administered is ##STR211##
 5. A method for treating a retroviral infection in a patient in need thereof comprising: administering to the patient a therapeutically effective amount of a napthol compound, or a pharmaceutically acceptable salt thereof, wherein the naphthol or salt administered is ##STR212##
 6. A compound having the structure where P is one or more counterions.
 7. A compound having the structure ##STR213## where P is one or more counterions.
 8. A compound having the structure ##STR214## where P is one or more counterions.
 9. A compound having the structure ##STR215## where P is one or more counterions.
 10. A compound having the structure ##STR216## where P is one or more counterions.
 11. A compound having the structure ##STR217## where P is one or more counterions.
 12. A compound having the structure ##STR218## where P is one or more counterions.
 13. A compound having the structure ##STR219## where P is one or more counterions. 